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抗原逆转确定了调理素化免疫球蛋白针对妊娠相关疟疾的靶标。

Antigen reversal identifies targets of opsonizing IgGs against pregnancy-associated malaria.

作者信息

Lambert Lester H, Bullock Jeanee L, Cook Sharma T, Miura Kazutoyo, Garboczi David N, Diakite Mahamadou, Fairhurst Rick M, Singh Kavita, Long Carole A

机构信息

Laboratory of Malaria and Vector Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, Maryland, USA.

Structural Biology Section, Research Technologies Branch, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, Maryland, USA.

出版信息

Infect Immun. 2014 Nov;82(11):4842-53. doi: 10.1128/IAI.02097-14. Epub 2014 Aug 25.

Abstract

Clinical immunity to pregnancy associated-malaria (PAM) in multigravida women has been attributed to antibodies that recognize VAR2CSA on the infected erythrocyte (IE) surface. The size and complexity of VAR2CSA have focused efforts on selecting one or more of its six Duffy binding-like (DBL) domains for vaccine development. Presently, however, there is no consensus as to which DBL domain(s) would be most effective in eliciting immunity. This is because antibodies to a number of the DBL domains have been found to block the adhesion of VAR2CSA-expressing erythrocytes to chondroitin sulfate A (CSA)-a major criterion for evaluating vaccine candidacy. Opsonization of IEs by cytophilic antibodies that recognize VAR2CSA represents an important yet understudied effector mechanism in acquired immunity to PAM. To date, no studies have sought to determine the targets of those antibodies. In this study, we found that IgGs from multigravida Malian women showed (i) higher reactivity to recombinant DBL domains by enzyme-linked immunosorbent assay (ELISA), (ii) more binding to VAR2CSA-expressing IEs, and (iii) greater opsonization of these IEs by human monocytic cells than IgGs from malaria-exposed Malian men and malaria-naive American adults. Preincubation of IgGs from multigravida women with recombinant DBL2χ, DBL3χ, or DBL5ε domains significantly diminished opsonization of VAR2CSA-expressing IEs by human monocytes. These data identify the DBL2χ, DBL3χ, and DBL5ε domains as the primary targets of opsonizing IgGs for the first time. Our study introduces a new approach to determining the antigenic targets of opsonizing IgGs in phagocytosis assays.

摘要

多孕妇女对妊娠相关疟疾(PAM)的临床免疫被认为归因于识别感染红细胞(IE)表面VAR2CSA的抗体。VAR2CSA的大小和复杂性使得疫苗开发工作集中在选择其六个达菲结合样(DBL)结构域中的一个或多个。然而,目前对于哪个DBL结构域在引发免疫方面最有效尚无共识。这是因为已发现针对多个DBL结构域的抗体可阻断表达VAR2CSA的红细胞与硫酸软骨素A(CSA)的粘附,而CSA粘附是评估疫苗候选性的主要标准。识别VAR2CSA的嗜细胞抗体对IE的调理作用是获得性PAM免疫中一种重要但未被充分研究的效应机制。迄今为止,尚无研究试图确定这些抗体的靶标。在本研究中,我们发现,与来自接触过疟疾的马里男性和未接触过疟疾的美国成年人的IgG相比,来自多孕马里妇女的IgG表现出:(i)通过酶联免疫吸附测定(ELISA)对重组DBL结构域的反应性更高;(ii)与表达VAR2CSA的IE结合更多;(iii)人单核细胞对这些IE的调理作用更强。用重组DBL2χ、DBL3χ或DBL5ε结构域对多孕妇女的IgG进行预孵育,可显著降低人单核细胞对表达VAR2CSA的IE的调理作用。这些数据首次确定DBL2χ、DBL3χ和DBL5ε结构域是调理IgG的主要靶标。我们的研究引入了一种在吞噬试验中确定调理IgG抗原靶标的新方法。

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